As cells enter mitosis, cell cortex contraction generates surface tension to establish a geometry feasible for division in a physically confined environment. Cell surface tension rises in prophase and continues to stay constant during metaphase to support mitosis. How the cell surface tension is maintained throughout mitosis is not well explored. We show that the cell surface tension is actively maintained by a mechanosensitive RhoA pathway at the cell cortex during mitosis. Mechanical activation of RhoA leads to non-muscle myosin IIB (NMIIB) stabilization and mechanosensitive accumulation at the cell cortex via Rho kinase (ROCK) regulation of the NMIIB head domain. Interestingly, when the NMIIB tail domain regulation is perturbed, the NMIIB has reduced ability to generate tension but could still support mitotic cells to withstand compressive stress by undergoing mechanosensitive accumulation at the cell cortex. Thus, mechanical RhoA activation drives NMIIB mechanoresponse via its head domain regulation to maintain cell surface tension during mitosis.
Mechanical properties of red blood cells (RBCs) change during their senescence which supports numerous physiological or pathological processes in circulatory systems by providing crucial cellular mechanical environments of hemodynamics. However, quantitative studies on the aging and variations of RBC properties are largely lacking. Herein, we investigate morphological changes, softening or stiffening of single RBCs during aging using an in vitro mechanical fatigue model. Using a microfluidic system with microtubes, RBCs are repeatedly subjected to stretch and relaxation as they squeeze into and out of a sudden contraction region. Geometric parameters and mechanical properties of healthy human RBCs are characterized systematically upon each mechanical loading cycle. Our experimental results identify three typical shape transformations of RBCs during mechanical fatigue, which are all strongly associated with the loss of surface area. We constructed mathematical models for the evolution of surface area and membrane shear modulus of single RBCs during mechanical fatigue, and quantitatively developed an ensemble parameter to evaluate the aging status of RBCs. This study provides not only a novel in vitro fatigue model for investigating the mechanical behavior of RBCs, but also an index closely related to the age and inherent physical properties for a quantitative differentiation of individual RBCs.
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